EP0214839B1 - Improvements in relation to drug treatments - Google Patents

Improvements in relation to drug treatments Download PDF

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Publication number
EP0214839B1
EP0214839B1 EP86306823A EP86306823A EP0214839B1 EP 0214839 B1 EP0214839 B1 EP 0214839B1 EP 86306823 A EP86306823 A EP 86306823A EP 86306823 A EP86306823 A EP 86306823A EP 0214839 B1 EP0214839 B1 EP 0214839B1
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Prior art keywords
fatty acid
porphyrins
porphyrin
formula
case
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German (de)
French (fr)
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EP0214839A2 (en
EP0214839A3 (en
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David Frederick C/O Efamol Ltd. Horrobin
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Efamol Holdings PLC
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/185Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
    • A61K31/19Carboxylic acids, e.g. valproic acid
    • A61K31/20Carboxylic acids, e.g. valproic acid having a carboxyl group bound to a chain of seven or more carbon atoms, e.g. stearic, palmitic, arachidic acids
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/40Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having five-membered rings with one nitrogen as the only ring hetero atom, e.g. sulpiride, succinimide, tolmetin, buflomedil
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/65Tetracyclines
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P31/00Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
    • A61P31/12Antivirals
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/10Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis

Definitions

  • the invention relates in one aspect to the reduction of undesired skin sensitivity to light in drug treatments and in another aspect to enhancement of the effect of treatment with porphyrins.
  • Certain drugs increase the sensitivity of the skin to light.
  • porphyrins tetracyclines and Benoxaprofen.
  • porphyrins used as tumour-locating agents followed by light irradiation to destroy the tumour cells, may require patients to remain in subdued light for some time to avoid generalised skin reactions.
  • Haematoporphyrin derivatives of unknown specific composition have been used in cancer treatment, having been found to localise in tumours in many tissues after injection into the bloodstream and to sensitise the diseased cells to light iradiation. No explanation for the absorption into tumour cells is known, but irradiated cells (unless pigmented) are rapidly killed to a depth depending on the light penetration. Attention has recently been drawn also to localisation in atheromatous tissue in arteries and also in virus infected cells, giving potential for their selective destruction also.
  • EP-A-0 186 962 discloses when for use in therapy or for the preparation of medicaments therefor, compounds essentially of the formula below. It also discloses methods of therapy, in particular of light-sensitive porphyrin absorbing tumours, making use of the compounds, namely: wherein, each R is an ortho, meta or para positioned hydroxy (-OH), amino (-NH2) or sulphhydryl (-SH) substituent optionally itself substituted for example by alkyl or acyl groups preferably C1 to C4. Substitution may be at some or all of the groups R.
  • the R groups and any substituents thereof may be the same or different and in the same or different positions on their respective substitutent rings, which may themselves be replaced by other aromatic ring systems.
  • nucleus or the substituent rings may be substituted further, provided pharmacological acceptability, appreciable solubility in water, absorption of light at the red end of the spectrum, and absorption by cancerous tissue are retained and the compounds when in such form are to be understood as included in the above formula.
  • Any of the compounds further may be in the form of derivatives such as addition salts at acidic or basic centres, or for example hydrates or other solvates particularly with lower aliphatic alcohols. It is preferred that one or more of the substituents R should be of a kind and in a form able to ionise at physiological pH, to increase the absorption in the red part of the spectrum, that is in the portion that most effectively penetrates tissue.
  • HK7 and other specific compounds are more effective photosensitisers for tumour tissue in animal assay than is HpD and (ii) that they do not cause detectable general cerebral photosensitivity in animals at doses producing substantial tumour sensitisation and, therefore, have promise in the treatment of brain tumours.
  • the present invention is a development of the use of haematoporphyrins and related compounds, particularly those to which EP-A-0 186 962 relates.
  • the present invention provides, based on administration of polyunsaturated fatty acids (polyunsaturates) in conjunction with (preferably before, during and after) the administration of the porphyrin and its light activation.
  • polyunsaturated fatty acids polyunsaturates
  • the present invention provides, based on administration of polyunsaturated fatty acids (polyunsaturates) in conjunction with (preferably before, during and after) the administration of the porphyrin and its light activation.
  • Separate administration will normally be convenient but compositions of polyunsaturates and porphyrins are not excluded from the scope of the invention.
  • Administration can be for any indication including cancer, atheroma and inactivation of viruses.
  • the invention also provides a method of preventing photosensitivity reactions in natural porphyrias in which the porphyrins are endogenously generated.
  • the invention thus lies in compositions comprising the drugs referred to in conjunction with polyunsaturates.
  • the invention lies also in compositions of the drugs and the polyunsaturates, for use where convenient, and in preparation of medicaments, being such compositions for such purpose.
  • polyunsaturates 1 mg to 500 g per day of the polyunsaturates, preferably 100 mg to 10 g, or molar equivalent amounts of derivatives as referred to below.
  • the polyunsaturates can be administered for days, weeks or even months prior to the drug, particularly light/porphyrin, treatment and continued for similar periods afterwards depending on the retention of the drug in the body (elimination of porphyrins is slow).
  • the drug treatment is itself conventional.
  • Ranges for the dose of illumination are, for example, 2.5 to 500 J/cm2 conveniently 5 to 250 J/cm2 depending primarily on tumour thickness. In some instances more than one such does of light may be desirable following a single, or possibly, more than one such administration of the porphyrin.
  • the polyunsaturates used are preferably the essential fatty acids of the n-6 and n-3 series.
  • the pathways of metabolism of the n-6 essential fatty acids and the related n-3 acids sharing, it is believed, common enzymes in the two pathways, are:
  • the pathways are not normally reversible nor, in man, are n-3 and n-6 series acids interconvertible.
  • the acids which naturally are of the all-cis configuration, are systematically named as derivatives of the corresponding octadecanoic, eicosanoic or docosanoic acids, e.g. delta-9,12-octadecadienoic acid or delta-4,7,10,13,16,19-docosahexaenoic acid, but numerical designation such as, correspondingly, 18:2 n-6 or 22:6 n-3 is convenient.
  • Initials for example DHA for 22:6 n-3 ( d ocosa h exaenoic a cid), are also used but do not serve when n-3 and n-6 acids of the same chain length and degree of unsaturation exist.
  • n-6 series Trivial names in more or less common use in the n-6 series are as shown. Of the n-3 series only 18:3 n-3 has a commonly used trivial name, alpha-linolenic acid. It was characterised earlier than gamma-linolenic acid and reference in the literature simply to linolenic acid, especially in the earlier literature is to the alpha-acid.
  • the acids may be used as such or as pharmaceutically acceptable and physiologically equivalent derivatives as, for example, detailed later herein for gamma-linolenic acid and dihomo-gamma-linolenic acid, and reference to any of the acids is to be taken as including reference to the acids when in the form of such derivatives.
  • Equivalence is demonstrated by entry into the pathways quoted herein, as evidenced by effects corresponding to those of the acids themselves or their natural glyceride esters.
  • indirect identification of useful derivatives is by their having the valuable effect in the body of the acid itself, but conversion can be shown directly by gas chromatographic analysis of concentrations in blood, body fat, or other tissue by standard techniques, for example those of Pelick et al. p. 23, "Analysis of Lipids and Lipoproteins" Ed. Perkins, American Oil Chemist Society, Champaign, Illinois, U.S.A.
  • packs may be prepared comprising the materials presented for separate, or part joint and part separate administration in the appropriate relative amounts, and use of such packs is within the purview of this invention.
  • Convenient physiologically equivalent derivatives of gamma-linolenic acid and dihomo-gamma-linolenic acid for use according to the invention, as with the other acids, include salts, amides, esters including glyceride esters and alkyl (e.g. C1 to C4) esters, and phospholipids.
  • salts include salts, amides, esters including glyceride esters and alkyl (e.g. C1 to C4) esters, and phospholipids.
  • compositions may be produced for use in the invention by associating the natural or synthetic acids, as such or as derivatives, with an acceptable pharmaceutical vehicle. It is, however, at present convenient to incorporate at least the gamma-linolenic acid into compositions in the form of an available oil having a high gamma-linolenic acid content, hence reference to "oil" herein.
  • oils having a high gamma-linolenic acid content are few (there are no known natural sources of significant amounts of dihomo-gamma-linolenic acid).
  • One source of oils currently available is the seed of Evening Primrose species such as Oenothera biennis L . and Oenothera lamarckiana , the oil extract therefrom containing gamma-linolenic acid (about 8%) and linoleic acid (about 72%) in the form of their glycerides together with other glycerides (percentages based on total fatty acids).
  • gamma-linolenic acid sources of gamma-linolenic acid are Borage species such as Borago officinalis which, though current yield per acre is low, provide a richer source of gamma-linolenic acid than Oenothera oil. Recent studies on fungi which can be cultivated by fermentation promise a fungal oil source.
  • the oil is extracted from the seed by one of the conventional methods of extraction such as cold pressure, screw pressure after partially cooking the seed, or solvent extraction.
  • seed oil extracts referred to above can be used as such or can, for example, if desired, be fractionated to yield an oily composition containing the triglycerides of gamma-linolenic and linoleic as the main fatty acid components, the gamma-linolenic acid content being if desired a major proportion. Seed oil extracts appear to have a stabilising effect upon dihomo-gamma-linolenic acid if present.
  • Natural sources of 22:4 and 22:5 n-6 acids include adrenal glands (22:5) and kidneys (22:4) obtained from slaughter houses, and 22:4 in the fat of the American Snapping Turtle.
  • the n-3 acids are available from fish oils, particularly 20:5 n-3 and 22:6 n-3.
  • the acids can be isolated from these sources by, for example, saponification under mild non-oxidising conditions followed by preparative gas liquid chromatography. Synthesis of the acids is difficult but not impossible and provides another source.
  • a preservative is incorporated into the preparations: alpha-tocopherol in conenctration of about 0.1% by weight has been found suitable for the purpose.
  • Soft gelatine capsules made by conventional methods are administered in conjunction with tetracycline, Benoxaprofen, HpD or KH7 treatment in doses conventional for such treatment or in the case of treatment with HK7 daily doses as set out in the published Application, in the preferred range of 0.25 - 1.0 mg/kg, as follows:
  • a pack as referred to herein comprises 500 mg capsules of Evening Primrose Oil as above, to be taken 6/day, together, for example, with HpD or HK7 treatment.
  • Treatment with HK7 may, for example, specifically be:

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  • Urology & Nephrology (AREA)
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Abstract

A composition comprises a polyunsaturated fatty acid, in particular an essential fatty acid of the n-6 series (linoleic acid or its metabolites) or the n-3 series (alpha-linolenic acid and its metabolites), together with a drug that taken alone has a side-effect of sensitising the skin to light, in particular a porphyrin or tetracycline or Benoxaprofen, alone or in a pharmaceutically acceptable diluent or carrier, the composition reducing that sensitisation.

Description

  • The invention relates in one aspect to the reduction of undesired skin sensitivity to light in drug treatments and in another aspect to enhancement of the effect of treatment with porphyrins.
  • Certain drugs increase the sensitivity of the skin to light. Among them are porphyrins, tetracyclines and Benoxaprofen. In particular, porphyrins, used as tumour-locating agents followed by light irradiation to destroy the tumour cells, may require patients to remain in subdued light for some time to avoid generalised skin reactions.
  • We have found that polyunsaturates, as specified later herein, counter these adverse sensitivities and may be given topically or systemically by ingestion or any other convenient means.
  • Haematoporphyrin derivatives of unknown specific composition (HpD, a mixture of tetrapyrroles derived from natural sources) have been used in cancer treatment, having been found to localise in tumours in many tissues after injection into the bloodstream and to sensitise the diseased cells to light iradiation. No explanation for the absorption into tumour cells is known, but irradiated cells (unless pigmented) are rapidly killed to a depth depending on the light penetration. Attention has recently been drawn also to localisation in atheromatous tissue in arteries and also in virus infected cells, giving potential for their selective destruction also.
  • In EP-A-0 186 962 published 9th July 1986, there are described improvements on HpD in relation to tumour treatment, based on well characterised and thus more exactly controllable compounds.
  • EP-A-0 186 962 discloses when for use in therapy or for the preparation of medicaments therefor, compounds essentially of the formula below. It also discloses methods of therapy, in particular of light-sensitive porphyrin absorbing tumours, making use of the compounds, namely:
    Figure imgb0001
    wherein, each R is an ortho, meta or para positioned hydroxy (-OH), amino (-NH₂) or sulphhydryl (-SH) substituent optionally itself substituted for example by alkyl or acyl groups preferably C₁ to C₄. Substitution may be at some or all of the groups R. The R groups and any substituents thereof may be the same or different and in the same or different positions on their respective substitutent rings, which may themselves be replaced by other aromatic ring systems. The nucleus or the substituent rings may be substituted further, provided pharmacological acceptability, appreciable solubility in water, absorption of light at the red end of the spectrum, and absorption by cancerous tissue are retained and the compounds when in such form are to be understood as included in the above formula. Any of the compounds further may be in the form of derivatives such as addition salts at acidic or basic centres, or for example hydrates or other solvates particularly with lower aliphatic alcohols. It is preferred that one or more of the substituents R should be of a kind and in a form able to ionise at physiological pH, to increase the absorption in the red part of the spectrum, that is in the portion that most effectively penetrates tissue.
  • It is noted further in EP-A-0 186 962 that methods of preparation of porphyrin compounds are known in the art and may be used for example to make a preferred compound, itself known, namely 5,10,15,20-tetra(4-hydroxyphenyl)porphyrin (HK7) which may be used as such or as its tetraethyl or tetra-acetyl derivatives. Reference to the published Application shall thus be made for the preparation and properties of the compounds of formula I.
  • Evidence is for example presented (i) that HK7 and other specific compounds are more effective photosensitisers for tumour tissue in animal assay than is HpD and (ii) that they do not cause detectable general cerebral photosensitivity in animals at doses producing substantial tumour sensitisation and, therefore, have promise in the treatment of brain tumours.
  • In one aspect, the present invention is a development of the use of haematoporphyrins and related compounds, particularly those to which EP-A-0 186 962 relates.
  • On exposure to adequate light intensity, these compounds are raised to an excited state and generate toxic substances such as singlet oxygen and related radicals. These materials thus damage cells which have taken up large amounts of porphyrin. Normal cells do, however, take up the compound and so can be damaged by light exposure. After administration of HpD or related compounds patients must therefore stay in subdued light for a period: otherwise they run the risk of developing severe skin inflammation similar to that which occurs in certain natural porphyrias.
  • It is thus advantageous to have a method of reducing the damage to normal tissue, which in its present aspect the present invention provides, based on administration of polyunsaturated fatty acids (polyunsaturates) in conjunction with (preferably before, during and after) the administration of the porphyrin and its light activation. Separate administration will normally be convenient but compositions of polyunsaturates and porphyrins are not excluded from the scope of the invention. Administration can be for any indication including cancer, atheroma and inactivation of viruses.
  • The invention also provides a method of preventing photosensitivity reactions in natural porphyrias in which the porphyrins are endogenously generated.
    • MODE OF ACTION WITH PORPHYRINS
  • In addition to protecting normal tissue effectiveness is believed to be related to promotion by polyunsaturates of the formation of superoxide and related radicals, which in cells involved in inflammatory reactions is itself known. By administering the polyunsaturates at a dose level adequate to provide some enrichment of malignant cells, those cells appear to generate toxic radicals more strongly on exposure to porphyrin and light than they would otherwise, with increase in the lethality to those cells of the porphyrin/light treatment of malignancy.
  • At first sight it is difficult to understand how a polyunsaturate could simultaneously protect normal cells from radiation damage and potentiate that damage in malignant cells. However, it is known that polyunsaturates are vital for the structure of cells and other membranes and for the normal regulation of prostaglandin and leukotriene biosynthesis. These desirable actions must be balanced against possible toxicity resulting from generation of superoxide and other radicals. We have repeatedly observed in cell culture experiments that human malignant cells are damaged by concentrations of polyunsaturated fatty acids which do not damage normal human fibroblasts, suggesting that malignant cells may be less able than normal ones to defend themselves against free radicals and other toxic materials which can be generated from polyunsaturated fatty acids. While we would not wish to be limited by the theory, we suggest that in normal cells the polyunsaturate effect on formation of free radicals and other toxic materials is effectively neutralised, leaving unopposed the important desirable effects of polyunsaturates on cell membranes and other structures, effects which stabilise the cell and reduce light-induced damage. In malignant cells, in contrast, for reasons which are as yet unclear, there appear to be inadequate defences against the polyunsaturate effects of promoting production of free radicals and other toxic substances, so that these toxic effects become predominant and enhance the damage produced by the porphyrin/light interaction.
  • Broadly therefore the effect of the administration of polyunsaturates prior to, during and after light/porphyrin therapy, is believed to be in potentiating the desired effects of that therapy as well as in reducing the side effects in normal tissues.
    • DRUGS GENERALLY
  • The mode of action in reduction of light sensitivity of the skin in use of the other drugs, such as tetracyclines, and of normal tissue in use of porphyrins, is less clear but may be due to an effect of these drugs in disturbing the normal bodily function of polyunsaturates reducing their effects so that supplementation is required.
    • THE INVENTION
  • The invention thus lies in compositions comprising the drugs referred to in conjunction with polyunsaturates. The invention lies also in compositions of the drugs and the polyunsaturates, for use where convenient, and in preparation of medicaments, being such compositions for such purpose.
    • DOSES
  • 1 mg to 500 g per day of the polyunsaturates, preferably 100 mg to 10 g, or molar equivalent amounts of derivatives as referred to below. The polyunsaturates can be administered for days, weeks or even months prior to the drug, particularly light/porphyrin, treatment and continued for similar periods afterwards depending on the retention of the drug in the body (elimination of porphyrins is slow). The drug treatment is itself conventional.
  • Dosages with the porphyrins of the published Application require a balance between doses being high enough to show useful necrosis and not so high as to be prohibitively toxic. For example, the lithium, sodium and zinc salts of HK7 show useful necrosis at 12.5 µmol/kg, µmol/kg = micromols, while HK7 itself is reasonably effective at 6.25 µmol/kg. We would expect the most effective does in man to lie in the range of 0.25 - 1.0 mg/kg subject to the fact that the safe and effective range for a given compound must be found by trial. At its widest, subject always to that proviso, the range will not be outside 0.01 to 10.0 (or possibly up to 100) mg/kg. Ranges for the dose of illumination are, for example, 2.5 to 500 J/cm² conveniently 5 to 250 J/cm² depending primarily on tumour thickness. In some instances more than one such does of light may be desirable following a single, or possibly, more than one such administration of the porphyrin.
    • SUITABLE POLYUNSATURATES
  • The polyunsaturates used are preferably the essential fatty acids of the n-6 and n-3 series.
  • The pathways of metabolism of the n-6 essential fatty acids and the related n-3 acids sharing, it is believed, common enzymes in the two pathways, are:
    Figure imgb0002
    The pathways are not normally reversible nor, in man, are n-3 and n-6 series acids interconvertible.
  • The acids, which naturally are of the all-cis configuration, are systematically named as derivatives of the corresponding octadecanoic, eicosanoic or docosanoic acids, e.g. delta-9,12-octadecadienoic acid or delta-4,7,10,13,16,19-docosahexaenoic acid, but numerical designation such as, correspondingly, 18:2 n-6 or 22:6 n-3 is convenient. Initials, for example DHA for 22:6 n-3 (docosahexaenoic acid), are also used but do not serve when n-3 and n-6 acids of the same chain length and degree of unsaturation exist. Trivial names in more or less common use in the n-6 series are as shown. Of the n-3 series only 18:3 n-3 has a commonly used trivial name, alpha-linolenic acid. It was characterised earlier than gamma-linolenic acid and reference in the literature simply to linolenic acid, especially in the earlier literature is to the alpha-acid.
  • The acids may be used as such or as pharmaceutically acceptable and physiologically equivalent derivatives as, for example, detailed later herein for gamma-linolenic acid and dihomo-gamma-linolenic acid, and reference to any of the acids is to be taken as including reference to the acids when in the form of such derivatives. Equivalence is demonstrated by entry into the pathways quoted herein, as evidenced by effects corresponding to those of the acids themselves or their natural glyceride esters. Thus, indirect identification of useful derivatives is by their having the valuable effect in the body of the acid itself, but conversion can be shown directly by gas chromatographic analysis of concentrations in blood, body fat, or other tissue by standard techniques, for example those of Pelick et al. p. 23, "Analysis of Lipids and Lipoproteins" Ed. Perkins, American Oil Chemist Society, Champaign, Illinois, U.S.A.
    • PACKS
  • If it is not desired to have compositions comprising the different active materials together, packs may be prepared comprising the materials presented for separate, or part joint and part separate administration in the appropriate relative amounts, and use of such packs is within the purview of this invention.
    • FORMS AND SOURCES OF GAMMA-LINOLENIC AND OTHER ACIDS
  • Convenient physiologically equivalent derivatives of gamma-linolenic acid and dihomo-gamma-linolenic acid for use according to the invention, as with the other acids, include salts, amides, esters including glyceride esters and alkyl (e.g. C₁ to C₄) esters, and phospholipids. As noted above, reference to the acids in the claims and elsewhere herein are to be taken as including them when in the form of said derivatives.
  • If desired, pharmaceutical compositions may be produced for use in the invention by associating the natural or synthetic acids, as such or as derivatives, with an acceptable pharmaceutical vehicle. It is, however, at present convenient to incorporate at least the gamma-linolenic acid into compositions in the form of an available oil having a high gamma-linolenic acid content, hence reference to "oil" herein.
  • At the present time known natural sources of oils having a high gamma-linolenic acid content are few (there are no known natural sources of significant amounts of dihomo-gamma-linolenic acid). One source of oils currently available is the seed of Evening Primrose species such as Oenothera biennis L. and Oenothera lamarckiana, the oil extract therefrom containing gamma-linolenic acid (about 8%) and linoleic acid (about 72%) in the form of their glycerides together with other glycerides (percentages based on total fatty acids). Other sources of gamma-linolenic acid are Borage species such as Borago officinalis which, though current yield per acre is low, provide a richer source of gamma-linolenic acid than Oenothera oil. Recent studies on fungi which can be cultivated by fermentation promise a fungal oil source.
  • The oil is extracted from the seed by one of the conventional methods of extraction such as cold pressure, screw pressure after partially cooking the seed, or solvent extraction.
  • Fractionation of a typical sample of this oil in the form of methyl esters shows the relative proportions:
    Figure imgb0003
  • The seed oil extracts referred to above can be used as such or can, for example, if desired, be fractionated to yield an oily composition containing the triglycerides of gamma-linolenic and linoleic as the main fatty acid components, the gamma-linolenic acid content being if desired a major proportion. Seed oil extracts appear to have a stabilising effect upon dihomo-gamma-linolenic acid if present.
  • Natural sources of 22:4 and 22:5 n-6 acids include adrenal glands (22:5) and kidneys (22:4) obtained from slaughter houses, and 22:4 in the fat of the American Snapping Turtle. The n-3 acids are available from fish oils, particularly 20:5 n-3 and 22:6 n-3.
  • The acids can be isolated from these sources by, for example, saponification under mild non-oxidising conditions followed by preparative gas liquid chromatography. Synthesis of the acids is difficult but not impossible and provides another source.
  • Advantageously, a preservative is incorporated into the preparations: alpha-tocopherol in conenctration of about 0.1% by weight has been found suitable for the purpose.
    • EXAMPLES
  • Soft gelatine capsules made by conventional methods are administered in conjunction with tetracycline, Benoxaprofen, HpD or KH7 treatment in doses conventional for such treatment or in the case of treatment with HK7 daily doses as set out in the published Application, in the preferred range of 0.25 - 1.0 mg/kg, as follows:
    • 1. 500 mg capsules of Evening Primrose Oil containing 45 mg gamma-linolenic acid, 6/day;
    • 2. 500 mg capsules of borage oil containing 90 mg gamma-linolenic acid, 4/day;
    • 3. 100 mg capsules of pure gamma-linolenic acid, 4/day;
    • 4. 50 mg capsules of pure dihomo-gamma-linolenic acid, 6/day;
    • 5. Capsules containing 100 mg gamma-linolenic acid, 20 mg 20:4 n-6, 50 mg 20:5 n-3, 5/day;
    • 6. Capsules containing 100 mg gamma-linolenic acid, 50 mg 22:4 n-6, 50 mg 20:5 n-3, 50 mg 22:6 n-3, 5/day.
  • A pack as referred to herein comprises 500 mg capsules of Evening Primrose Oil as above, to be taken 6/day, together, for example, with HpD or HK7 treatment.
  • Treatment with HK7 may, for example, specifically be:
    • 1. Administer, for 14 days prior to injection of the porphyrin, 8 capsules per day of 80% Evening Primrose Oil and 20% fish oil (as a source of 20:5 and 22:6 n-3 acids);
    • 2. Administer the porphyrin at 12.5 µmol/kg and after the appropriate interval expose the tissue to laser irradiation while continuing the administration of the polyunsaturates;
    • 3. Continue administration of the polyunsaturates for 8 weeks after laser irradiation.

Claims (14)

  1. A method for the preparation of a composition having the effect of reducing the sensitisation of the skin to light normally associated with a drug that taken alone has a side effect of sensitising the skin to light, comprising: mixing (i) a polyunsaturated fatty acid; and (ii) a drug that taken alone has a side effect of sensitising the skin to light and optionally a pharmaceutically acceptable diluent or carrier.
  2. A method as in claim 1, wherein the drug used is selected from a porphyrin, a tetracycline or Benoxaprofen.
  3. A method as in claim 2, wherein the porphyrin is HpD or a pharmacologically acceptable and water soluble meso-porphyrin of the formula:
    Figure imgb0005
     where n = 1 to 3 and each substituent R, the same or different and at the same or different point in its respective substituent phenyl ring or other aromatic group replacing the ring, is a hydroxy, amino or sulphhydryl group.
  4. A method according to any of claims 1 to 3, wherein the composition is prepared in dosage units suited to administration of 1 mg to 500 g of the fatty acid daily, and in the case of porphyrins generally or Benoxaprofen a conventional daily dose, and in the case of porphyrins according to formula I as set out in claim 3 a pharmacologically acceptable and effective amount within the range 0,01 to 100 mg/kg (based on a 70 kg adult).
  5. A method for the preparation of a medicament for use in conjunction with a drug that taken alone has a side effect of sensitising the skin to light or for use in ameliorating the effects of spontaneous porphyrias, characterised in that said medicament is prepared in a form that comprises a polyunsaturated fatty acid.
  6. A method as in claim 5, wherein the drug is selected from a porphyrin, a tetracycline or Benoxaprofen.
  7. A method according to claim 6, wherein the porphyrin is HpD or a porphyrin according to formula I as set out in claim 3.
  8. A method according to any of claims 5 to 7, wherein the amounts of said materials are 1 mg to 500 g of the fatty acid daily, and in the case of porphyrins according to formula I as set out in claim 3 a pharmacologically acceptable and effective amount within the range 0,01 to 100 mg/kg (based on a 70 kg adult).
  9. A method for the preparation of a composition suited for administration and subsequent light irradiation to destroy tumour or atheromatous or virus infected cells comprising mixing: (i) a polyunsaturated acid; and (ii) HpD or other tumour locating porphyrin including porphyrins according to formula I as set out in claim 3, and optionally a pharmaceutically acceptable diluent or carrier.
  10. A method according to claim 9, wherein the composition is prepared in dosage units suited to administration of 1 mg to 500 g of the fatty acid daily, and in the case of porphyrins generally a conventional daily amount, and in the case of porphyrins according to formula I as set out in claim 3 a pharmacologically acceptable and effective amount within the range 0,01 to 100 mg/kg (based on a 70 kg adult).
  11. A method for the preparation of a medicament for use in enhancing the effect of administered tumour or atheromatous or virus infected cell locating porphyrins in subsequent light irradiation to destroy said cells, characterised in that said medicament is prepared in a form that comprises a polyunsaturated fatty acid.
  12. A method according to claim 11, wherein the amounts of said materials are 1 mg to 500 g of the fatty acid daily, and in the case of porphyrins generally a conventional daily amount, and in the case of porphyrins according to formula I as set out in claim 3 a pharmacologically acceptable and effective amount within the range 0,01 to 100 mg/kg (based on a 70 kg adult).
  13. A method as claimed in any of claims 5, 6, 7, 8, 11 and 12 wherein the polyunsaturated fatty acid is an essential fatty acid of the n-6 series (linoleic acid or its metabolites) or the n-3 series (alpha-linolenic acid and its metabolites) optionally with a pharmaceutically acceptable diluent or carrier.
  14. A method as claimed in any of claims 1, 2, 3, 4, 9 and 10, wherein the polyunsaturated fatty acid is an essential fatty acid of the n-6 series (linoleic acid or its metabolites) or the n-3 series (alpha-linolenic acid and its metabolites).
EP86306823A 1985-09-13 1986-09-03 Improvements in relation to drug treatments Expired - Lifetime EP0214839B1 (en)

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US5599840A (en) * 1986-11-26 1997-02-04 Bar Ilan University Physiologically active and nutritional composition
GB8805849D0 (en) * 1988-03-11 1988-04-13 Efamol Holdings Porphyrins & cancer treatment
IL91802A (en) * 1988-10-27 1994-05-30 Univ Bar Ilan Compositions containing linolenic acid derivativesfor treating Alzheimer's disease, related dementias and epilepsy
US5219878A (en) * 1990-10-05 1993-06-15 Queen's University Tetrapyrrole hydroxyalkylamide photochemotherapeutic agents
GB9301446D0 (en) * 1993-01-26 1993-03-17 Scotia Holdings Plc Internal radiation damage
US5368841A (en) * 1993-02-11 1994-11-29 The General Hospital Corporation Photodynamic therapy for the destruction of the synovium in the treatment of rheumatoid arthritis and the inflammatory arthritides
US5639460A (en) * 1995-06-07 1997-06-17 Raymond; Hal C. Aqueous plant extract having antiviral activity
US7112609B2 (en) * 1999-06-01 2006-09-26 Drugtech Corporation Nutritional supplements
FR2860720A1 (en) * 2003-10-09 2005-04-15 Jean Pascal Conduzorgues NOVEL PHARMACEUTICAL COMPOSITIONS FOR TREATING XEROSTOMY AND SIMILAR DISEASES
GB0907413D0 (en) 2009-04-29 2009-06-10 Equateq Ltd Novel methods
US8293790B2 (en) 2011-10-19 2012-10-23 Dignity Sciences Limited Pharmaceutical compositions comprising DGLA and benzoyl peroxide and methods of use thereof
KR102391827B1 (en) 2014-06-04 2022-04-27 디에스 바이오파마 리미티드 Pharmaceutical compositions comprising dgla and use of same
US20210315851A1 (en) 2020-04-03 2021-10-14 Afimmune Limited Compositions comprising 15-hepe and methods of treating or preventing hematologic disorders, and/or related diseases

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DE3681667D1 (en) 1991-10-31
EP0214839A2 (en) 1987-03-18
GB8522670D0 (en) 1985-10-16
CA1275249C (en) 1990-10-16
US5589509A (en) 1996-12-31
IE862351L (en) 1987-03-13
ZA866743B (en) 1987-04-29
EP0214839A3 (en) 1989-01-25
ATE67676T1 (en) 1991-10-15
US4996233A (en) 1991-02-26
JPS6267021A (en) 1987-03-26
AU592593B2 (en) 1990-01-18
JP2588390B2 (en) 1997-03-05
AU6255486A (en) 1987-03-19
IE59001B1 (en) 1993-12-15

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